Combining laboratory and mathematical models to infer mechanisms underlying kinetic changes in macrophage susceptibility to an RNA virus.

Andrea Doeschl-WilsonAlison WilsonJens NielsenHans NauwynckAlan ArchibaldTahar Ait-Ali

Published in: BMC systems biology (2016)

Our dynamic model-inference approach provides strong support that PAM susceptibility to the PRRS virus is transient, reversible and can be mediated by compounds produced by the target cells themselves, and that these can render PAMs lacking the CD163 receptor susceptible to PRRSV. The results have implications for the development of therapeutics aiming to boost target cell resistance and prompt future investigation of dynamic changes in macrophage susceptibility to PRRSV and other viruses.

Keyphrases

single cell
induced apoptosis
adipose tissue
cell cycle arrest
current status
small molecule
endoplasmic reticulum stress
cell proliferation
mesenchymal stem cells
brain injury
disease virus